COMMENTARY ON THE LAW

Genetic factors in pathogenesis, course and treatment of inflammatory bowel diseases

Hubert Zatorski¹ , Maciej Sałaga¹ , Marta Zielińska¹ , Jakub Fichna¹

1. Zakład Biochemii, Wydział Lekarski, Uniwersytet Medyczny w Łodzi

Published: 2015-03-17

DOI: 10.5604/17322693.1145172

GICID: 01.3001.0009.6508

Available language versions: en pl

Issue: Postepy Hig Med Dosw 2015; 69 : 335-344

Abstract

Inflammatory bowel diseases (IBD) are a group of chronic gastrointestinal disorders with alternating relapses and remissions. Two main types within IBD can be distinguished: Crohn’s disease and ulcerative colitis. Considering the epidemiological, immunological and genetic data, it was concluded that IBD possess multifactorial etiology, where genetic and environmental factors form the immunological background for the disease. In this review we discuss the most important genes and their protein products in IBD etiology and their impact on IBD pharmacotherapy.

References

1. Amre D.K., Mack D.R., Morgan K., Krupoves A., Costea I., LambretteP., Grimard G., Dong J., Feguery H., Bucionis V., DeslandresC., Levy E., Seidman E.G.: Autophagy gene ATG16L1 but not IRGMis associated with Crohn’s disease in Canadian children. Inflamm.Bowel Dis., 2009; 15: 501-507
Google Scholar
2. Barreiro M., Nunez C., Dominguez-Munoz J.E., Lorenzo A., BarreiroF., Potel J., Pena A.S.: Association of NOD2/CARD15 mutationswith previous surgical procedures in Crohn’s disease. Rev. Esp. Enferm.Dig., 2005; 97: 547-553
Google Scholar
3. Barreiro-de Acosta M., Pena A.S.: Clinical applications of NOD2/CARD15 mutations in Crohn’s disease. Acta Gastroenterol. Latinoam.,2007; 37: 49-54
Google Scholar
4. Barrett J.C., Hansoul S., Nicolae D.L. Cho J.H., Duerr R.H., RiouxJ.D., Brant S.R., Silverberg M.S., Taylor K.D., Barmada M.M., Bitton A.,Dassopoulos T., Datta L.W., Green T., Griffiths A.M. i wsp.: Genomewideassociation defines more than 30 distinct susceptibility loci forCrohn’s disease. Nat. Genet., 2008; 40: 955-962
Google Scholar
5. Bekpen C., Marques-Bonet T., Alkan C., Antonacci F., LeograndeM.B., Ventura M., Kidd J.M., Siswara P., Howard J.C., Eichler E.E.:Death and resurrection of the human IRGM gene. PLoS Genet., 2009;5: e1000403
Google Scholar
6. Brand S., Staudinger T., Schnitzler F., Pfennig S., Hofbauer K.,Dambacher J., Seiderer J., Tillack C., Konrad A., Crispin A., Goke B.,Lohse P., Ochsenkuhn T.: The role of Toll-like receptor 4 Asp299Gly and Thr399Ile polymorphisms and CARD15/NOD2 mutations in thesusceptibility and phenotype of Crohn’s disease. Inflamm. BowelDis., 2005; 11: 645-652
Google Scholar
7. Brest P., Lapaquette P., Souidi M., Lebrigand K., Cesaro A., VouretCraviariV., Mari B., Barbry P., Mosnier J.F., Hebuterne X., HarelBellanA., Mograbi B., Darfeuille-Michaud A., Hofman P.: A synonymousvariant in IRGM alters a binding site for miR-196 and causesderegulation of IRGM-dependent xenophagy in Crohn’s disease. Nat.Genet., 2011; 43: 242-245
Google Scholar
8. Cadwell K., Liu J.Y., Brown S.L., Miyoshi H., Loh J., Lennerz J.K.,Kishi C., Kc W., Carrero J.A., Hunt S., Stone C.D., Brunt E.M., XavierR.J., Sleckman B.P., Li E., Mizushima N., Stappenbeck T.S., Virgin H.W.4th: A key role for autophagy and the autophagy gene Atg16l1 inmouse and human intestinal Paneth cells. Nature, 2008; 456: 259-263
Google Scholar
9. Cario E.: Toll-like receptors in inflammatory bowel diseases: a decadelater. Inflamm. Bowel Dis., 2010; 16: 1583-1597
Google Scholar
10. Cario E., Rosenberg I.M., Brandwein S.L., Beck P.L., ReineckerH.C., Podolsky D.K.: Lipopolysaccharide activates distinct signalingpathways in intestinal epithelial cell lines expressing Toll-like receptors.J. Immunol., 2000; 164: 966-972
Google Scholar
11. Chan I., Liu L., Hamada T., Sethuraman G., McGrath J.A.: The molecularbasis of lipoid proteinosis: mutations in extracellular matrixprotein 1. Exp. Dermatol., 2007; 16: 881-890
Google Scholar
12. Cheng J.F., Ning Y.J., Zhang W., Lu Z.H., Lin L.: T300A polymorphismof ATG16L1 and susceptibility to inflammatory bowel diseases:a meta-analysis. World J. Gastroenterol., 2010; 16: 1258-1266
Google Scholar
13. Cruikshank W.W., Kornfeld H., Center D.M.: Interleukin-16. J.Leukoc. Biol., 2000; 67: 757-766
Google Scholar
14. Cuffari C.: The genetics of inflammatory bowel disease: diagnosticand therapeutic implications. World J. Pediatr., 2010; 6: 203-209
Google Scholar
15. Dey I., Lejeune M., Chadee K.: Prostaglandin E2 receptor distributionand function in the gastrointestinal tract. Br. J. Pharmacol.,2006; 149: 611-623
Google Scholar
16. Duerr R.H., Taylor K.D., Brant S.R., Rioux J.D., Silverberg M.S.,Daly M.J., Steinhart A.H., Abraham C., Regueiro M., Griffiths A., DassopoulosT., Bitton A., Yang H., Targan S., Datta L.W. i wsp.: A genomewideassociation study identifies IL23R as an inflammatory boweldisease gene. Science, 2006; 314: 1461-1463
Google Scholar
17. El-Tawil A.M.: Jews and inflammatory bowel disease. J. Gastrointestin.Liver Dis., 2009; 18: 137-138
Google Scholar
18. Fisher S.A., Tremelling M., Anderson C.A., Gwilliam R., BumpsteadS., Prescott N.J., Nimmo E.R., Massey D., Berzuini C., JohnsonC., Barrett J.C., Cummings F.R., Drummond H., Lees C.W., Onnie C.M.I wsp.: Genetic determinants of ulcerative colitis include the ECM1locus and five loci implicated in Crohn’s disease. Nat. Genet., 2008;40: 710-712
Google Scholar
19. Franchimont D., Vermeire S., El Housni H., Pierik M., Van SteenK., Gustot T., Quertinmont E., Abramowicz M., Van Gossum A.,Deviere J., Rutgeerts P.: Deficient host-bacteria interactions in inflammatorybowel disease? The toll-like receptor (TLR)-4 Asp299glypolymorphism is associated with Crohn’s disease and ulcerativecolitis. Gut, 2004; 53: 987-992
Google Scholar
20. Fujita N., Itoh T., Omori H., Fukuda M., Noda T., Yoshimori T.:The Atg16L complex specifies the site of LC3 lipidation for membranebiogenesis in autophagy. Mol. Biol. Cell., 2008; 19: 2092-2100
Google Scholar
21. Fujiya M., Inaba Y., Musch M.W., Hu S., Kohgo Y., Chang E.B.:Cytokine regulation of OCTN2 expression and activity in small andlarge intestine. Inflamm. Bowel Dis., 2011; 17: 907-916
Google Scholar
22. Gardet A., Benita Y., Li C., Sands B.E., Ballester I., Stevens C.,Korzenik J.R., Rioux J.D., Daly M.J., Xavier R.J., Podolsky D.K.: LRRK2is involved in the IFN-γ response and host response to pathogens.J. Immunol., 2010; 185: 5577-5585
Google Scholar
23. Glas J., Seiderer J., Bues S., Stallhofer J., Fries C., Olszak T., TsekeriE., Wetzke M., Beigel F., Steib C., Friedrich M., Göke B., Diegelmann J.,Czamara D., Brand S.: IRGM variants and susceptibility to inflammatorybowel disease in the German population. PLoS One, 2013; 8: e54338
Google Scholar
24. Glas J., Seiderer J., Czamara D., Pasciuto G., Diegelmann J., WetzkeM., Olszak T., Wolf C., Müller-Myhsok B., Balschun T., AchkarJ.P., Kamboh M.I., Franke A., Duerr R.H., Brand S.: PTGER4 expression-modulatingpolymorphisms in the 5p13.1 region predisposeto Crohn’s disease and affect NF-κB and XBP1 binding sites. PLoSOne, 2012; 7: e52873
Google Scholar
25. Glas J., Seiderer J., Wetzke M., Konrad A., Török H.P., SchmechelS., Tonenchi L., Grassl C., Dambacher J., Pfennig S., Maier K., GrigaT., Klein W., Epplen J.T., Schiemann U. i wsp.: rs1004819 is the maindisease-associated IL23R variant in German Crohn’s disease patients:combined analysis of IL23R, CARD15, and OCTN1/2 variants. PLoSOne, 2007; 2: e819
Google Scholar
26. Glas J., Torok H.P., Unterhuber H., Radlmayr M., Folwaczny C.:The -295T-to-C promoter polymorphism of the IL-16 gene is associatedwith Crohn’s disease. Clin. Immunol., 2003; 106: 197-200
Google Scholar
27. Halfvarson J., Bodin L., Tysk C., Lindberg E., Jarnerot G.: Inflammatorybowel disease in a Swedish twin cohort: a long-term followupof concordance and clinical characteristics. Gastroenterology,2003; 124: 1767-1773
Google Scholar
28. Halme L., Paavola-Sakki P., Turunen U., Lappalainen M., FarkkilaM., Kontula K.: Family and twin studies in inflammatory boweldisease. World J. Gastroenterol., 2006; 12: 3668-3672
Google Scholar
29. Hampe J., Schreiber S., Shaw S.H., Lau K.F., Bridger S., MacphersonA.J., Cardon L.R., Sakul H., Harris T.J., Buckler A., Hall J., StokkersP., van Deventer S.J., Nürnberg P., Mirza M.M. i wsp.: A genomewideanalysis provides evidence for novel linkages in inflammatorybowel disease in a large European cohort. Am. J. Hum. Genet.,1999; 64: 808-816
Google Scholar
30. Hart A.L., Al-Hassi H.O., Rigby R.J., Bell S.J., Emmanuel A.V.,Knight S.C., Kamm M.A., Stagg A.J.: Characteristics of intestinal dendriticcells in inflammatory bowel diseases. Gastroenterology, 2005;129: 50-65
Google Scholar
31. Hausmann M., Kiessling S., Mestermann S., Webb G., Spottl T.,Andus T., Scholmerich J., Herfarth H., Ray K., Falk W., Rogler G.: Tolllikereceptors 2 and 4 are up-regulated during intestinal inflammation.Gastroenterology, 2002; 122: 1987-2000
Google Scholar
32. Kabi A., Nickerson K.P., Homer C.R., McDonald C.: Digesting thegenetics of inflammatory bowel disease: insights from studies of autophagyrisk genes. Inflamm. Bowel Dis., 2012; 18: 782-792
Google Scholar
33. Keates A.C., Castagliuolo I., Cruickshank W.W., Qiu B., ArseneauK.O., Brazer W., Kelly C.P.: Interleukin 16 is up-regulated in Crohn’sdisease and participates in TNBS colitis in mice. Gastroenterology,2000; 119: 972-982
Google Scholar
34. Kett L.R., Dauer W.T.: Leucine-rich repeat kinase 2 for beginners:six key questions. Cold Spring Harb. Perspect. Med., 2012; 2: a009407
Google Scholar
35. Laberge S., Ernst P., Ghaffar O., Cruikshank W.W., Kornfeld H.,Center D.M., Hamid Q.: Increased expression of interleukin-16 inbronchial mucosa of subjects with atopic asthma. Am. J. Respir. CellMol. Biol., 1997; 17: 193-202
Google Scholar
36. Langholz E.: Current trends in inflammatory bowel disease: thenatural history. Ther. Adv. Gastroenterol., 2010; 3: 77-86
Google Scholar
37. Latiano A., Annese V.: Genetics and ulcerative colitis: what arethe clinical implications? Curr. Drug Targets, 2011; 12: 1383-1389
Google Scholar
38. Latiano A., Palmieri O., Cucchiara S., Castro M., D’Inca R., GuarisoG., Dallapiccola B., Valvano M.R., Latiano T., Andriulli A., Annese V.:Polymorphism of the IRGM gene might predispose to fistulizing behaviorin Crohn’s disease. Am. J. Gastroenterol., 2009; 104: 110-116
Google Scholar
39. Lees C.W., Barrett J.C., Parkes M., Satsangi J.: New IBD genetics:common pathways with other diseases. Gut, 2011; 60: 1739-1753
Google Scholar
40. Lovato P., Brender C., Agnholt J., Kelsen J., Kaltoft K., SvejgaardA., Eriksen K.W., Woetmann A., Odum N.: Constitutive STAT3 activationin intestinal T cells from patients with Crohn’s disease. J. Biol.Chem., 2003; 278: 16777-16781
Google Scholar
41. Mathy N.L., Bannert N., Norley S.G., Kurth R.: Cutting edge:CD4 is not required for the functional activity of IL-16. J. Immunol.,2000; 164: 4429-4432
Google Scholar
42. Matsuda A., Suzuki Y., Honda G., Muramatsu S., Matsuzaki O.,Nagano Y., Doi T., Shimotohno K., Harada T., Nishida E., Hayashi H.,Sugano S.: Large-scale identification and characterization of humangenes that activate NF-κB and MAPK signaling pathways. Oncogene,2003; 22: 3307-3318
Google Scholar
43. McGovern D., Powrie F.: The IL23 axis plays a key role in thepathogenesis of IBD. Gut, 2007; 56: 1333-1336
Google Scholar
44. Murphy S.F., Kwon J.H., Boone D.L.: Novel players in inflammatorybowel disease pathogenesis. Curr. Gastroenterol. Rep., 2012; 14: 146-152
Google Scholar
45. Okazaki T., Wang M.H., Rawsthorne P., Sargent M., Datta L.W.,Shugart Y.Y., Bernstein C.N., Brant S.R.: Contributions of IBD5, IL23R,ATG16L1, and NOD2 to Crohn’s disease risk in a population-basedcase-control study: evidence of gene-gene interactions. Inflamm.Bowel Dis., 2008; 14: 1528-1541
Google Scholar
46. Palomino-Morales R.J., Oliver J., Gomez-Garcia M., Lopez-NevotM.A., Rodrigo L., Nieto A., Alizadeh B.Z., Martin J.: Association ofATG16L1 and IRGM genes polymorphisms with inflammatory boweldisease: a meta-analysis approach. Genes Immun., 2009; 10: 356-364
Google Scholar
47. Podolsky D.K., Gerken G., Eyking A., Cario E.: Colitis-associatedvariant of TLR2 causes impaired mucosal repair because of TFF3deficiency. Gastroenterology, 2009; 137: 209-220
Google Scholar
48. Rumio C., Besusso D., Palazzo M., Selleri S., Sfondrini L., DubiniF., Menard S., Balsari A.: Degranulation of paneth cells via toll-likereceptor 9. Am. J. Pathol., 2004; 165: 373-381
Google Scholar
49. Seegert D., Rosenstiel P., Pfahler H., Pfefferkorn P., Nikolaus S.,Schreiber S.: Increased expression of IL-16 in inflammatory boweldisease. Gut, 2001; 48: 326-332
Google Scholar
50. Shih D.Q., Targan S.R., McGovern D.: Recent advances in IBDpathogenesis: genetics and immunobiology. Curr. Gastroenterol.Rep., 2008; 10: 568-575
Google Scholar
51. Silverberg M.S.: OCTNs: will the real IBD5 gene please stand up?World J. Gastroenterol., 2006; 12: 3678-3681
Google Scholar
52. Singh S.B., Davis A.S., Taylor G.A., Deretic V.: Human IRGM inducesautophagy to eliminate intracellular mycobacteria. Science,2006; 313: 1438-1441
Google Scholar
53. Sonne S., Shekhawat P.S., Matern D., Ganapathy V., IgnatowiczL.: Carnitine deficiency in OCTN2-/- newborn mice leads to a severegut and immune phenotype with widespread atrophy, apoptosis anda pro-inflammatory response. PLoS One, 2012; 7: e47729
Google Scholar
54. Stoll M., Corneliussen B., Costello C.M., Waetzig G.H., MellgardB., Koch W.A., Rosenstiel P., Albrecht M., Croucher P.J., Seegert.D,Nikolaus S., Hampe J., Lengauer T., Pierrou S., Foelsch U.R., MathewC.G., Lagerstrom-Fermer M., Schreiber S.: Genetic variation in DLG5is associated with inflammatory bowel disease. Nat. Genet., 2004;36: 476-480
Google Scholar
55. Strober W., Watanabe T.: NOD2, an intracellular innate immunesensor involved in host defense and Crohn’s disease. Mucosal Immunol.,2011; 4: 484-495
Google Scholar
56. Sugimoto K.: Role of STAT3 in inflammatory bowel disease.World J. Gastroenterol., 2008; 14: 5110-5114
Google Scholar
57. Takafuji V.A., Evans A., Lynch K.R., Roche J.K.: PGE2 receptors andsynthesis in human gastric mucosa: perturbation in cancer. ProstaglandinsLeukot. Essent. Fatty Acids, 2002; 66: 71-81
Google Scholar
58. Taylor K.D., Targan S.R., Mei L., Ippoliti A.F., McGovern D.,Mengesha E., King L., Rotter J.I.: IL23R haplotypes provide a largepopulation attributable risk for Crohn’s disease. Inflamm. Bowel.Dis., 2008; 14: 1185-1191
Google Scholar
59. Tong Y., Yamaguchi H., Giaime E., Boyle S., Kopan R., KelleherR.J., III, Shen J.: Loss of leucine-rich repeat kinase 2 causes impairmentof protein degradation pathways, accumulation of α-synuclein,and apoptotic cell death in aged mice. Proc. Natl. Acad. Sci. USA,2010; 107: 9879-9884
Google Scholar
60. Tsianos E.V., Katsanos K.H., Tsianos V.E.: Role of genetics in thediagnosis and prognosis of Crohn›s disease. World J. Gastroenterol.,2012; 18: 105-118
Google Scholar
61. Urcelay E., Mendoza J.L., Martinez A., Fernandez L., Taxonera C.,Diaz-Rubio M., de la Concha E.G.: IBD5 polymorphisms in inflammatorybowel disease: association with response to infliximab. WorldJ. Gastroenterol., 2005; 11: 1187-1192
Google Scholar
62. Vaz F.M., Scholte H.R., Ruiter J., Hussaarts-Odijk L.M., PereiraR.R., Schweitzer S., de Klerk J.B., Waterham H.R., Wanders R.J.: Identificationof two novel mutations in OCTN2 of three patients with systemiccarnitine deficiency. Hum. Genet., 1999; 105: 157-161
Google Scholar
63. Vermeire S.: Genetic susceptibility and application of genetictesting in clinical management of inflammatory bowel disease. Aliment.Pharmacol. Ther., 2006; 24, Suppl. 3: 2-10
Google Scholar
64. Wehkamp J., Harder J., Weichenthal M., Schwab M., Schaffeler E.,Schlee M., Herrlinger K.R., Stallmach A., Noack F., Fritz P., SchroderJ.M., Bevins C.L., Fellermann K., Stange E.F.: NOD2 (CARD15) mutationsin Crohn’s disease are associated with diminished mucosalα-defensin expression. Gut, 2004; 53: 1658-1664
Google Scholar
65. Weiss B., Lebowitz O., Fidder H.H., Maza I., Levine A., ShaoulR., Reif S., Bujanover Y., Karban A.: Response to medical treatmentin patients with Crohn›s disease: the role of NOD2/CRAD15,disease phenotype, and age of diagnosis. Dig. Dis. Sci., 2010; 55:1674-1680
Google Scholar
66. Wu X., Prasad P.D., Leibach F.H., Ganapathy V.: cDNA sequence,transport function, and genomic organization of human OCTN2,a new member of the organic cation transporter family. Biochem.Biophys. Res. Commun., 1998; 246: 589-595
Google Scholar
67. Zhou L., Ivanov I.I., Spolski R., Min R., Shenderov K., Egawa T.,Levy D.E., Leonard W.J., Littman D.R.: IL-6 programs TH-17 cell differentiationby promoting sequential engagement of the IL-21 andIL-23 pathways. Nat. Immunol., 2007; 8: 967-974
Google Scholar

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